Ibalizumab Plus Optimized Background Regimen in Patient With Multi-Drug Resistant HIV

Phase 3

Completed

Conditions: HIV

Interventions: Biological: ibalizumab
Drug: Optimized Background Regimen (OBR)

Registration Number: NCT02475629

Lead Sponsor: TaiMed Biologics Inc.

Brief Summary: This Phase 3, single arm, multicenter study will evaluate the safety and effectiveness of ibalizumab in treatment-experienced patients infected with multi-drug resistant HIV-1.

Detailed Description: This Phase 3, single arm, multicenter study will evaluate the safety and effectiveness of ibalizumab in treatment-experienced patients infected with multi-drug resistant HIV-1. Patients must have been treated with HAART for at least 6 months and be failing or have recently failed (i.e., in the last 8 weeks) therapy to determine baseline viral load.

Days 0-6 of the study will be a "control period." During Days 0 through 6 patients will be monitored on current failing therapy (or no therapy, if the patient has failed and discontinued treatment within the 8 weeks preceding Screening).

Days 7-13 of the study will be an "essential monotherapy period." During Days 7 through 13 patients will continue on current failing therapy and receive one 2000 mg dose (loading dose) of ibalizumab on Day 7. Day 7 is Baseline for the treatment period (Day 7-Week 25).

Day 14-Week 25 of the study will be the "maintenance period." On Day 14 (primary endpoint), the OBR will be initiated and must include at least one agent to which the patient's virus is susceptible. Beginning at Day 21, 800 mg of ibalizumab will be administered every 2 weeks through Week 23.

End of Study evaluations will be performed at Week 25, and a follow-up visit will be conducted at Week 29.

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 40

Inclusion Criteria

Are capable of understanding and have voluntarily signed the informed consent document
Have documented HIV-1 infection by official, signed, written history (e.g., laboratory report), otherwise an HIV-antibody test will be performed
Have no acquired immunodeficiency syndrome (AIDS)-defining events in the 3 months before Screening, other than cutaneous Kaposi's sarcoma or wasting syndrome due to HIV
Are able and willing to comply with all protocol requirements and procedures
Have a life expectancy that is >6 months.
Have a viral load >1,000 copies/mL and documented resistance to at least one antiretroviral medication from each of three classes of antiretroviral medications as measured by resistance testing
Have a history of at least 6 months on antiretroviral treatment
Are receiving a stable highly active antiretroviral regimen for at least 8 weeks before Screening and are willing to continue that regimen until Day 14, OR (in the past 8 weeks) have failed and are off therapy and are willing to stay off therapy until Day 14
Have full viral sensitivity/susceptibility to at least one antiretroviral agent, other than ibalizumab, as determined by the screening resistance tests and be willing and able to be treated with at least one agent to which the patient's viral isolate is fully sensitive/susceptible according to the screening resistance tests as a component of OBR
If sexually active, are willing to use an effective method of contraception during the study and for 30 days after the last administration of the study drug

Exclusion Criteria

Any active AIDS-defining illness per Category C conditions according to the Centers for Disease Control and Prevention (CDC) Classification System for HIV Infection, with the following exceptions: cutaneous Kaposi's sarcoma and wasting syndrome due to HIV
Any significant diseases (other than HIV-1 infection) or clinically significant findings, including psychiatric and behavioral problems, determined from screening, medical history and/or physical examination that, in the investigator's opinion, would preclude the patient from participating in this study
Any significant acute illness within 1 week before the initial administration of study drug
Any active infection secondary to HIV requiring acute therapy; however, patients that require maintenance therapy (i.e., secondary prophylaxis for opportunistic infections) will be eligible for the study.
Any immunomodulating therapy (including interferon), systemic steroids, or systemic chemotherapy within 12 weeks before Enrollment
Any prior exposure to ibalizumab (formerly TNX-355 and Hu5A8)
Any vaccination within 7 days before Enrollment
Any female patient who either is pregnant, intends to become pregnant, or is currently breastfeeding
Any current alcohol or illicit drug use that, in the investigator's opinion, will interfere with the patient's ability to comply with the study schedule and protocol evaluations
Any previous clinically significant allergy or hypersensitivity to any excipient in the ibalizumab formulation
Any radiation therapy during the 28 days before first administration of investigational medication
Any Grade 3 or 4 laboratory abnormality according to the Division of AIDS grading scale, except for the following asymptomatic Grade 3 events triglyceride elevation total cholesterol elevation

Study & Design

Study Type: INTERVENTIONAL

Study Design: SINGLE_GROUP

Arm && Interventions

Group	Intervention	Description
Open-Label Ibalizumab plus OBR	ibalizumab	2000 mg intravenous ibalizumab (loading dose) on Day 7 followed in 14 days (on Day 21) by 800 mg intravenous ibalizumab administered once every two weeks, plus an Optimized Background Regimen (OBR) beginning on Day 14.
Open-Label Ibalizumab plus OBR	Optimized Background Regimen (OBR)	2000 mg intravenous ibalizumab (loading dose) on Day 7 followed in 14 days (on Day 21) by 800 mg intravenous ibalizumab administered once every two weeks, plus an Optimized Background Regimen (OBR) beginning on Day 14.

Primary Outcome Measures

Name	Time	Method
Efficacy: Proportion of Participants Achieving a Viral Load Reduction of at Least 0.5 Log 10: ITT-MEF	Day 14	Proportion of participants (%) achieving a viral load reduction of at least 0.5 log from baseline (Day 7)
Efficacy: Proportion of Subjects With a Viral Load Decrease of at Least 0.5 Log 10 - Protocol Correct	Day 14	Proportion of patients (%) with a viral load decrease of at least 0.5 log 10 from baseline (day 7)

Secondary Outcome Measures

Name	Time	Method
End of Study Viral Load Reductions as a Measure of Efficacy - Protocol Correct Analysis	at Week 25/End of Study	Proportion of patients achieving a \>/= 0.5 log10 and \>/= 1.0 log10 decrease from Day 7/Baseline in viral load at Week 25/End of Study
Efficacy: Proportion of Patients With Undetectable Viral Load: ITT-MEF	Week 25 /end of study	Proportion of patients with undetectable Viral Load (\<50 copies/mL, and \<400 copies/mL)
Efficacy: Proportion of Patients With Undetectable HIV-RNA Levels: Protocol Correct	Week 25/End of Study	Proportion of patients (%) with HIV-RNA levels \< 50 copies/mL and \< 400 copies/mL at Week 25/End of Study
Mean Change in Viral Load as a Measure of Efficacy - ITT-MEF	Day 7 and Day 14	Mean change from Day 7/Baseline in log 10 vial load measured at Day 14
Mean Change in Viral Load as a Measure of Efficacy - Protocol Correct	Day 7 and Day 14	Mean change from Day 7/Baseline in Log 10 viral load measured at Day 14
End of Study Viral Load Reductions as a Measure of Efficacy - Intent to Treat Analysis	at Week 25/End of Study	Proportion of patients achieving a \>/= 0.5 log10 and \>/= 1.0 log10 decrease from Day 7/Baseline in viral load at Week 25/End of Study
Mean Change in CD4+ Cell Count as a Measure of Efficacy and Safety - ITT	Day 7 and Week 25/End of Study	Mean change from Day 7/Baseline in CD4+ cell count at Week 25/End of Study
Mean Change in CD4+ Cell Count as a Measure of Efficacy and Safety - Protocol Correct	Day 7 and Week 25/End of Study	Mean change from Day 7/Baseline in CD4+ cell count at Week 25/End of Study
Safety: Proportion of Participants Experiencing Adverse Events	Through Week 25/End of Study	Proportion of participants experiencing at least one treatment emergent adverse event to week 25/End of Study
Proportion of Participants Experiencing Adverse Event Related to Study Drug as a Measure of Safety and Tolerability	Through Week 25/End of Study	Proportion of participants experiencing a treatment emergent adverse event determined by the investigator to be related to study drug
Proportion of Participants Experiencing Serious Adverse Event as a Measure of Safety and Tolerability	Through Week 25/End of Study	Proportion of participants experiencing at least one serious treatment emergent adverse event, excluding death
Proportion of Participants Discontinuing Study Drug Due to Adverse Event	Through Week 25/End of Study	Proportion of participants discontinuing study drug due to occurrence of treatment emergent adverse event
Proportion of Participants Experiencing Adverse Event Grade 3 and Higher as a Measure of Safety and Tolerability	Through Week 25/End of Study	Proportion of participants experiencing treatment emergent adverse event Grade 3 and higher
Proportion of Participants Experiencing Adverse Event With Death as Outcome as a Measure of Safety and Tolerability	Through Week 25/End of Study	Proportion of participants experiencing treatment emergent adverse event with death as the outcome, regardless of relationship to study drug
Proportion of Participants Experiencing New AIDS-defining Adverse Event According to CDC Criteria as a Measure of Safety and Tolerability	Through Week 25/End of Study	Proportion of participants experiencing treatment emergent adverse event that is AIDS-defining by the CDC adverse event classification criteria for HIV infection

Trial Locations

Locations (30): University of Maryland, Institute of Human Virology
🇺🇸
Baltimore, Maryland, United States
Research Access Network
🇺🇸
Houston, Texas, United States
W King Health Care Group
🇺🇸
Los Angeles, California, United States
Midway Immunology and Research Center
🇺🇸
Fort Pierce, Florida, United States
Anthony Mills, MD, Inc.
🇺🇸
Los Angeles, California, United States
Triple O Research Institute
🇺🇸
West Palm Beach, Florida, United States
St. John Hospital and Medical Center
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Southfield, Michigan, United States
Georgetown University School of Medicine
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Washington, District of Columbia, United States
Henry Ford Health Systems
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Detroit, Michigan, United States
Gary Richmond, MD, PA
🇺🇸
Fort Lauderdale, Florida, United States
AIDS Research Consortium of Atlanta
🇺🇸
Atlanta, Georgia, United States
Clinical Research PR, Inc
🇵🇷
San Juan, Puerto Rico
Kaiser Foundation Research Institute
🇺🇸
San Francisco, California, United States
University of Miami
🇺🇸
Miami, Florida, United States
Long Beach Education and Research Consultants
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Long Beach, California, United States
Southern California Permanente Medical Group
🇺🇸
Los Angeles, California, United States
Ruane Medical and Clinical Research Institute
🇺🇸
Los Angeles, California, United States
Charles R. Drew Univ. of Med. & Science Clinical and Translational Research Center
🇺🇸
Los Angeles, California, United States
Quest Clinical Research
🇺🇸
San Francisco, California, United States
Orlando Immunology Center
🇺🇸
Orlando, Florida, United States
ACRIA
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New York, New York, United States
North Texas Infectious Disease Consultants
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Dallas, Texas, United States
Carolinas HealthCare System
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Charlotte, North Carolina, United States
Circle Care Center, LLC
🇺🇸
Norwalk, Connecticut, United States
Palmtree Clinical Research Inc.
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Palm Springs, California, United States
National Taiwan University Hospital
🇨🇳
Taipei, Taiwan
Yale University
🇺🇸
New Haven, Connecticut, United States
E-Da Hospital
🇨🇳
Kaohsiung, Taiwan
Montefiore Medical Center
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Bronx, New York, United States
AIDS Healthcare Foundation
🇺🇸
Los Angeles, California, United States